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Dive into the research topics where Alex Cortez is active.

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Featured researches published by Alex Cortez.


Science Translational Medicine | 2014

Rational design of small molecules as vaccine adjuvants

Manmohan Singh; Andrew T. Miller; Francesco Doro; David Skibinski; M. Lamine Mbow; Simone Bufali; Ann E. Herman; Alex Cortez; Yongkai Li; Bishnu P. Nayak; Elaine Tritto; Christophe M. Filippi; Gillis Otten; Luis A. Brito; Elisabetta Monaci; Chun Li; Susanna Aprea; Sara Valentini; Donatello Laera; Brunella Brunelli; Elena Caproni; Padma Malyala; Rekha G. Panchal; Travis K. Warren; Sina Bavari; Derek O'hagan; Michael P. Cooke; Nicholas M. Valiante

Small-molecule immune potentiators can be engineered to be potent adjuvants with localized innate immune activation and short in vivo residence times. Better Adjuvants Through Chemistry Vaccine development has come a long way since Jenner first noticed that cowpox protected against smallpox. And yet, many vaccines do not work well alone; adjuvants are included with the vaccine to boost the immune response. Despite the critical role of adjuvants in vaccine efficacy, new adjuvant development has been empirical. Now, Wu et al. report the rational optimization of small-molecule immune potentiators (SMIPs) as adjuvants. These SMIPs were engineered to have limited bioavailability and remain localized, inducing temporally and spatially restricted inflammation. This systematic approach to optimizing adjuvant properties may allow for improved immune responses to vaccines with fewer side effects. Adjuvants increase vaccine potency largely by activating innate immunity and promoting inflammation. Limiting the side effects of this inflammation is a major hurdle for adjuvant use in vaccines for humans. It has been difficult to improve on adjuvant safety because of a poor understanding of adjuvant mechanism and the empirical nature of adjuvant discovery and development historically. We describe new principles for the rational optimization of small-molecule immune potentiators (SMIPs) targeting Toll-like receptor 7 as adjuvants with a predicted increase in their therapeutic indices. Unlike traditional drugs, SMIP-based adjuvants need to have limited bioavailability and remain localized for optimal efficacy. These features also lead to temporally and spatially restricted inflammation that should decrease side effects. Through medicinal and formulation chemistry and extensive immunopharmacology, we show that in vivo potency can be increased with little to no systemic exposure, localized innate immune activation and short in vivo residence times of SMIP-based adjuvants. This work provides a systematic and generalizable approach to engineering small molecules for use as vaccine adjuvants.


Journal of Medicinal Chemistry | 2016

Incorporation of Phosphonate into Benzonaphthyridine Toll-like Receptor 7 Agonists for Adsorption to Aluminum Hydroxide

Alex Cortez; Yongkai Li; Andrew Todd Miller; Xiaoyue Zhang; Kathy Yue; Jillian Maginnis; Janice Hampton; De Shon Hall; Michael J. Shapiro; Bishnu P Nayak; Ugo D’Oro; Chun Li; David Skibinski; M. Lamine Mbow; Manmohan Singh; Derek T. O’Hagan; Michael P. Cooke; Nicholas M. Valiante; Tom Y.‐H. Wu

Small molecule Toll-like receptor 7 (TLR7) agonists have been used as vaccine adjuvants by enhancing innate immune activation to afford better adaptive response. Localized TLR7 agonists without systemic exposure can afford good adjuvanticity, suggesting peripheral innate activation (non-antigen-specific) is not required for immune priming. To enhance colocalization of antigen and adjuvant, benzonaphthyridine (BZN) TLR7 agonists are chemically modified with phosphonates to allow adsorption onto aluminum hydroxide (alum), a formulation commonly used in vaccines for antigen stabilization and injection site deposition. The adsorption process is facilitated by enhancing aqueous solubility of BZN analogs to avoid physical mixture of two insoluble particulates. These BZN-phosphonates are highly adsorbed onto alum, which significantly reduced systemic exposure and increased local retention post injection. This report demonstrates a novel approach in vaccine adjuvant design using phosphonate modification to afford adsorption of small molecule immune potentiator (SMIP) onto alum, thereby enhancing co-delivery with antigen.


Archive | 2011

Formulation of immunopotentiators

Manmohan Singh; David Skibinski; Tom Yao-Hsiang Wu; Yongkai Li; Alex Cortez; Xiaoyue Zhang; Yefen Zou; Timothy Z. Hoffman; Jianfeng Pan; Kathy Yue


Archive | 2017

CONJUGADOS DE ANTICUERPO QUE COMPRENDEN UN AGONISTA DEL RECEPTOR TIPO TOLL

Alex Cortez; Tom Yao Wu; Xing Hsiang Wnag; Tetsuo Uno; Shailaja Kasibhatla; Timothy Z. Hoffman; Bernhard Hubert Geierstanger


Archive | 2017

compostos e composições como moduladores da atividade de tlr

Alex Cortez; David Skibinski; Kathy Yue; Manmohan Singh; Tom Yao-Hsiang Wu; Xiaoyue Zhang; Yongkai Li


Archive | 2016

Conjugués d'anticorps comprenant un agoniste du récepteur de type toll

Alex Cortez; Bernhard Hubert Geierstanger; Timothy Z. Hoffman; Shailaja Kasibhatla; Tetsuo Uno; Xing Wang; Tom Yao-Hsiang Wu


Archive | 2011

Adsorption d'immunopotentiateurs sur des sels métalliques insolubles

Manmohan Singh; David Skibinski; Tom Yao-Hsiang Wu; Yefen Zou; Yongkai Li; Alex Cortez; Xiaoyue Zhang; Timothy Z. Hoffman; Jianfeng Pan; Kathy Yue


Archive | 2011

Adsorption von Immunpotentiatoren auf unlöslichen Metallsalzen

Manmohan Singh; David Skibinski; Tom Yao-Hsiang Wu; Yefen Zou; Yongkai Li; Alex Cortez; Xiaoyue Zhang; Timothy Z. Hoffman; Jianfeng Pan; Kathy Yue


Archive | 2011

Adsorption d'immunopotentialisateurs en sels métalliques insolubles

Alex Cortez; Timothy Z. Hoffman; Yongkai Li; Jianfeng Pan; Manmohan Singh; David Skibinski; Tom Yao-Hsiang Wu; Kathy Yue; Xiaoyue Zhang; Yefen Zou


Archive | 2010

Composés et compositions utilisés en tant que modulateurs de l'activité tlr

Alex Cortez; Yongkai Li; Manmohan Singh; David Skibinski; Tom Yao-Hsiang Wu; Kathy Yue; Xiaoyue Zhang

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Yongkai Li

Genomics Institute of the Novartis Research Foundation

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